Literature DB >> 28424285

Equine Arteritis Virus Has Specific Tropism for Stromal Cells and CD8+ T and CD21+ B Lymphocytes but Not for Glandular Epithelium at the Primary Site of Persistent Infection in the Stallion Reproductive Tract.

Mariano Carossino1, Alan T Loynachan2, Igor F Canisso3, R Frank Cook1, Juliana R Campos1, Bora Nam1, Yun Young Go1,4, Edward L Squires1, Mats H T Troedsson1, Thomas Swerczek1, Fabio Del Piero5, Ernest Bailey1, Peter J Timoney1, Udeni B R Balasuriya6.   

Abstract

Equine arteritis virus (EAV) has a global impact on the equine industry as the causative agent of equine viral arteritis (EVA), a respiratory, systemic, and reproductive disease of equids. A distinctive feature of EAV infection is that it establishes long-term persistent infection in 10 to 70% of infected stallions (carriers). In these stallions, EAV is detectable only in the reproductive tract, and viral persistence occurs despite the presence of high serum neutralizing antibody titers. Carrier stallions constitute the natural reservoir of the virus as they continuously shed EAV in their semen. Although the accessory sex glands have been implicated as the primary sites of EAV persistence, the viral host cell tropism and whether viral replication in carrier stallions occurs in the presence or absence of host inflammatory responses remain unknown. In this study, dual immunohistochemical and immunofluorescence techniques were employed to unequivocally demonstrate that the ampulla is the main EAV tissue reservoir rather than immunologically privileged tissues (i.e., testes). Furthermore, we demonstrate that EAV has specific tropism for stromal cells (fibrocytes and possibly tissue macrophages) and CD8+ T and CD21+ B lymphocytes but not glandular epithelium. Persistent EAV infection is associated with moderate, multifocal lymphoplasmacytic ampullitis comprising clusters of B (CD21+) lymphocytes and significant infiltration of T (CD3+, CD4+, CD8+, and CD25+) lymphocytes, tissue macrophages, and dendritic cells (Iba-1+ and CD83+), with a small number of tissue macrophages expressing CD163 and CD204 scavenger receptors. This study suggests that EAV employs complex immune evasion mechanisms that warrant further investigation.IMPORTANCE The major challenge for the worldwide control of EAV is that this virus has the distinctive ability to establish persistent infection in the stallion's reproductive tract as a mechanism to ensure its maintenance in equid populations. Therefore, the precise identification of tissue and cellular tropism of EAV is critical for understanding the molecular basis of viral persistence and for development of improved prophylactic or treatment strategies. This study significantly enhances our understanding of the EAV carrier state in stallions by unequivocally identifying the ampullae as the primary sites of viral persistence, combined with the fact that persistence involves continuous viral replication in fibrocytes (possibly including tissue macrophages) and T and B lymphocytes in the presence of detectable inflammatory responses, suggesting the involvement of complex viral mechanisms of immune evasion. Therefore, EAV persistence provides a powerful new natural animal model to study RNA virus persistence in the male reproductive tract.
Copyright © 2017 American Society for Microbiology.

Entities:  

Keywords:  EAV; EVA; arterivirus; cellular tropism; equine arteritis virus; equine viral arteritis; immune response; immunohistochemistry; male reproductive tract; persistent infection

Mesh:

Year:  2017        PMID: 28424285      PMCID: PMC5469258          DOI: 10.1128/JVI.00418-17

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  111 in total

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Review 4.  The molecular biology of arteriviruses.

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6.  Equine viral arteritis in newborn foals: clinical, pathological, serological, microbiological and immunohistochemical observations.

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Journal:  Equine Vet J       Date:  1997-05       Impact factor: 2.888

7.  Equine arteritis virus derived from an infectious cDNA clone is attenuated and genetically stable in infected stallions.

Authors:  U B Balasuriya; E J Snijder; L C van Dinten; H W Heidner; W D Wilson; J F Hedges; P J Hullinger; N J MacLachlan
Journal:  Virology       Date:  1999-07-20       Impact factor: 3.616

8.  Canine leukocyte integrins: characterization of a CD18 homologue.

Authors:  P F Moore; P V Rossitto; D M Danilenko
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9.  Genetic characterization of equine arteritis virus during persistent infection of stallions.

Authors:  Udeni B R Balasuriya; Jodi F Hedges; Victoria L Smalley; Andrea Navarrette; William H McCollum; Peter J Timoney; Eric J Snijder; N James MacLachlan
Journal:  J Gen Virol       Date:  2004-02       Impact factor: 3.891

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  8 in total

1.  Equine Arteritis Virus Elicits a Mucosal Antibody Response in the Reproductive Tract of Persistently Infected Stallions.

Authors:  Mariano Carossino; Bettina Wagner; Alan T Loynachan; R Frank Cook; Igor F Canisso; Lakshman Chelvarajan; Casey L Edwards; Bora Nam; John F Timoney; Peter J Timoney; Udeni B R Balasuriya
Journal:  Clin Vaccine Immunol       Date:  2017-10-05

2.  Downregulation of MicroRNA eca-mir-128 in Seminal Exosomes and Enhanced Expression of CXCL16 in the Stallion Reproductive Tract Are Associated with Long-Term Persistence of Equine Arteritis Virus.

Authors:  Mariano Carossino; Pouya Dini; Theodore S Kalbfleisch; Alan T Loynachan; Igor F Canisso; Kathleen M Shuck; Peter J Timoney; R Frank Cook; Udeni B R Balasuriya
Journal:  J Virol       Date:  2018-04-13       Impact factor: 5.103

3.  Intrahost Selection Pressure Drives Equine Arteritis Virus Evolution during Persistent Infection in the Stallion Reproductive Tract.

Authors:  Bora Nam; Zelalem Mekuria; Mariano Carossino; Ganwu Li; Ying Zheng; Jianqiang Zhang; R Frank Cook; Kathleen M Shuck; Juliana R Campos; Edward L Squires; Mats H T Troedsson; Peter J Timoney; Udeni B R Balasuriya
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5.  Perturbation of Thymocyte Development Underlies the PRRS Pandemic: A Testable Hypothesis.

Authors:  John E Butler; Marek Sinkora; Gang Wang; Katerina Stepanova; Yuming Li; Xuehui Cai
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6.  Equine arteritis virus long-term persistence is orchestrated by CD8+ T lymphocyte transcription factors, inhibitory receptors, and the CXCL16/CXCR6 axis.

Authors:  Mariano Carossino; Pouya Dini; Theodore S Kalbfleisch; Alan T Loynachan; Igor F Canisso; R Frank Cook; Peter J Timoney; Udeni B R Balasuriya
Journal:  PLoS Pathog       Date:  2019-07-29       Impact factor: 6.823

7.  Development of a TaqMan® Allelic Discrimination qPCR Assay for Rapid Detection of Equine CXCL16 Allelic Variants Associated With the Establishment of Long-Term Equine Arteritis Virus Carrier State in Stallions.

Authors:  Come J Thieulent; Mariano Carossino; Udeni B R Balasuriya; Kathryn Graves; Ernest Bailey; John Eberth; Igor F Canisso; Frank M Andrews; Michael L Keowen; Yun Young Go
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  8 in total

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